Global Patent Index - EP 3760730 A1

EP 3760730 A1 20210106 - METHODS FOR NON-INVASIVE PRENATAL PLOIDY CALLING

Title (en)

METHODS FOR NON-INVASIVE PRENATAL PLOIDY CALLING

Title (de)

VERFAHREN ZUR NICHTINVASIVEN PRÄNATALEN PLOIDIEZUORDNUNG

Title (fr)

PROCÉDÉS POUR UNE CLASSIFICATION DE PLOÏDIE PRÉNATALE NON INVASIVE

Publication

EP 3760730 A1 20210106 (EN)

Application

EP 20176621 A 20111118

Priority

  • US 201161462972 P 20110209
  • US 201161448547 P 20110302
  • US 201161516996 P 20110412
  • US 201113110685 A 20110518
  • US 201161571248 P 20110623
  • US 201161542508 P 20111003
  • EP 17150875 A 20111118
  • EP 14195468 A 20111118
  • EP 11858061 A 20111118
  • US 201113300235 A 20111118
  • US 2011061506 W 20111118

Abstract (en)

The present disclosure provides methods for determining the ploidy status of a chromosome in a gestating fetus from genotypic data measured from a mixed sample of DNA comprising DNA from both the mother of the fetus and from the fetus, and optionally from genotypic data from the mother and father. The ploidy state is determined by using a joint distribution model to create a plurality of expected allele distributions for different possible fetal ploidy states given the parental genotypic data, and comparing the expected allelic distributions to the pattern of measured allelic distributions measured in the mixed sample, and choosing the ploidy state whose expected allelic distribution pattern most closely matches the observed allelic distribution pattern. The mixed sample of DNA may be preferentially enriched at a plurality of polymorphic loci in a way that minimizes the allelic bias, for example using massively multiplexed targeted PCR.

IPC 8 full level

C12Q 1/68 (2018.01); G16B 20/10 (2019.01); G16B 20/20 (2019.01)

CPC (source: EP US)

C12Q 1/6827 (2013.01 - EP); C12Q 1/686 (2013.01 - EP); C12Q 1/6869 (2013.01 - EP); C12Q 1/6883 (2013.01 - EP US); G16B 20/00 (2019.01 - EP); G16B 20/10 (2019.01 - EP US); G16B 20/20 (2019.01 - EP US); G16H 10/40 (2017.12 - EP US); C12Q 1/6886 (2013.01 - EP); C12Q 2600/156 (2013.01 - EP); C12Q 2600/16 (2013.01 - EP)

C-Set (source: EP)

  1. C12Q 1/6827 + C12Q 2537/161 + C12Q 2537/165
  2. C12Q 1/686 + C12Q 2527/113 + C12Q 2527/143 + C12Q 2537/143 + C12Q 2537/165
  3. C12Q 1/686 + C12Q 2521/501 + C12Q 2525/155 + C12Q 2525/191 + C12Q 2537/143 + C12Q 2563/179
  4. C12Q 1/686 + C12Q 2535/122 + C12Q 2537/143 + C12Q 2563/179

Citation (applicant)

  • US 7888017 B2 20110215 - QUAKE STEPHEN [US], et al
  • US 60340609 P
  • US 2007184467 A1 20070809 - RABINOWITZ MATTHEW [US], et al
  • US 7634808 A 20080317
  • US 2008243398 A1 20081002 - RABINOWITZ MATTHEW [US], et al
  • US 2009052730 W 20090804
  • WO 2010017214 A1 20100211 - GENE SECURITY NETWORK INC [US], et al
  • US 2010050824 W 20100930
  • WO 2011041485 A1 20110407 - GENE SECURITY NETWORK INC [US], et al
  • US 201113110685 A 20110518
  • US 8008018 B2 20110830 - QUAKE STEPHEN [US], et al
  • US 7332277 B2 20080219 - DHALLAN RAVINDER S [US]
  • IB 2009052730 W 20090302
  • LIAO ET AL., CLIN. CHEM., vol. 57, no. 1, 2011, pages 92 - 101
  • PORRECA ET AL., NATURE METHODS, vol. 4, no. 11, 2007, pages 931 - 936
  • TURNER ET AL., NATURE METHODS, vol. 6, no. 5, 2009, pages 315 - 316
  • H. MAMON ET AL.: "Preferential Amplification of Apoptotic DNA from Plasma: Potential for Enhancing Detection of Minor DNA Alterations in Circulating DNA", CLINICAL CHEMISTRY, vol. 54, 2008, pages 9
  • A. SIKORA: "Detection of increased amounts of cell-free fetal DNA with short PCR amplicons", CLIN CHEM., vol. 56, no. 1, January 2010 (2010-01-01), pages 136 - 8, XP055081573, DOI: 10.1373/clinchem.2009.132951
  • WANG HYLUO MTERESHCHENKO IVFRIKKER DMCUI XLI JYHU GCHU YAZARO MALIN Y, GENOME RES., vol. 15, no. 2, February 2005 (2005-02-01), pages 276 - 83
  • LI HWANG HYCUI XLUO MHU GGREENAWALT DMTERESHCHENKO IVLI JYCHU YGAO R, METHODS MOL BIOL., 2007, pages 396
  • VARLEY KEMITRA RD, GENOME RES., vol. 18, no. 11, November 2008 (2008-11-01), pages 1844 - 50
  • G.J. W. LIAO ET AL., CLINICAL CHEMISTRY, vol. 57, no. 1, 2011, pages 92 - 101
  • FAN ET AL., PNAS, vol. 105, no. 42, 2008, pages 16266 - 16271
  • CHIU ET AL., BMJ, vol. 342, 2011, pages c7401

Citation (search report)

  • [A] WO 2007147074 A2 20071221 - LIVING MICROSYSTEMS INC [US], et al
  • [A] WO 03031646 A1 20030417 - UNIV QUEENSLAND [AU], et al
  • [A] GARY J W LIAO ET AL: "Targeted massively parallel sequencing of maternal plasma DNA permits efficient and unbiased detection of fetal alleles", vol. 57, no. 1, 1 January 2011 (2011-01-01), pages 92 - 101, XP002674771, ISSN: 0009-9147, Retrieved from the Internet <URL:http://www.clinchem.org/content/57/1/92> [retrieved on 20101115], DOI: 10.1373/CLINCHEM.2010.154336
  • [A] SHEN ZHIYONG ET AL: "MPprimer: a program for reliable multiplex PCR primer design", BMC BIOINFORMATICS, BIOMED CENTRAL, LONDON, GB, vol. 11, no. 1, 18 March 2010 (2010-03-18), pages 143, XP021071487, ISSN: 1471-2105, DOI: 10.1186/1471-2105-11-143
  • [A] JANNINE BROWNIE ET AL: "The elimination of primer-dimer accumulation in PCR", NUCLEIC ACIDS RESEARCH, OXFORD UNIVERSITY PRESS, GB, vol. 25, no. 16, 1 January 2007 (2007-01-01), pages 3235 - 3241, XP008156793, ISSN: 0305-1048
  • [A] MARKOULATOS P ET AL: "MULTIPLEX POLYMERASE CHAIN REACTION: A PRACTICAL APPROACH", JOURNAL OF CLINICAL LABORATORY ANALYSIS, NEW YORK, NY, US, vol. 16, no. 1, 1 January 2002 (2002-01-01), pages 47 - 51, XP009003351, ISSN: 0887-8013, DOI: 10.1002/JCLA.2058

Designated contracting state (EPC)

AL AT BE BG CH CY CZ DE DK EE ES FI FR GB GR HR HU IE IS IT LI LT LU LV MC MK MT NL NO PL PT RO RS SE SI SK SM TR

DOCDB simple family (publication)

EP 2902500 A1 20150805; EP 2902500 B1 20170111; EP 3187597 A1 20170705; EP 3187597 B1 20200603; EP 3760730 A1 20210106; EP 3760731 A1 20210106; EP 3760732 A1 20210106

DOCDB simple family (application)

EP 14195468 A 20111118; EP 17150875 A 20111118; EP 20176621 A 20111118; EP 20176629 A 20111118; EP 20176652 A 20111118